针对cMet受体构建的溶瘤腺病毒载体的特性

IF 6.7
Hany Sakr, D. T. Coleman, J. Cardelli, J. Mathis
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引用次数: 5

摘要

cMet受体是一种具有酪氨酸激酶活性的二聚体。在其配体肝细胞生长因子(HGF)的刺激下,受体介导广泛的生理作用。HGF-cMet信号通路在许多癌症中失调,这使得cMet成为新型治疗干预的重要靶点。溶瘤腺病毒(Ads)作为一种很有前景的治疗方法在过去的三十年中被广泛应用于多种肿瘤疾病。迄今为止,通过病毒基因组缺失或结合肿瘤选择性启动子来实现溶瘤性ad的癌症特异性复制。为了获得过表达cMet的癌细胞的溶瘤性Ad感染的新特异性,我们将HGF NK2序列插入到Ad血清型5 (Ad5)纤维基因中,该序列与HGF与cMet受体结合的竞争性拮抗剂相对应。得到的载体Ad5-pIX-RFP-FF/NK2被提取,在HEK293细胞中扩增,并进行表征。在表达不同水平的cMet和hCAR (Ad5受体)的各种癌细胞系中测试了结合特异性和病毒感染性。我们发现Ad5-pIX-RFP-FF/NK2对cMet受体具有结合特异性。此外,与非靶向Ad载体相比,病毒传染性和病毒复制能力增强。虽然NK2弱诱导cMet受体激活,但我们的结果显示在溶瘤性Ad病毒中没有受体磷酸化。综上所述,这些结果表明,重靶向cMet受体的溶瘤性Ad是开发新型癌症治疗剂的有希望的载体。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Characterization of an oncolytic adenovirus vector constructed to target the cMet receptor
The cMet receptor is a homodimer with tyrosine kinase activity. Upon stimulation with its ligand, hepatocyte growth factor (HGF), the receptor mediates wide physiologic actions. The HGF-cMet signaling pathway is dysregulated in many cancers, which makes cMet an important target for novel therapeutic interventions. Oncolytic adenoviruses (Ads) have been used for the past three decades as a promising therapeutic approach for a wide array of neoplastic diseases. To date, achieving cancer-specific replication of oncolytic Ads has been accomplished by either viral genome deletions or by incorporating tumor selective promoters. To achieve novel specificity of oncolytic Ad infection of cancer cells that overexpress cMet, we inserted the HGF NK2 sequence, corresponding to a competitive antagonist of HGF binding to the cMet receptor, into the Ad serotype 5 (Ad5) fiber gene. The resulting vector, Ad5-pIX-RFP-FF/NK2, was rescued, amplified in HEK293 cells, and characterized. Binding specificity and viral infectivity were tested in various cancer cell lines that express varying levels of cMet and hCAR (the Ad5 receptor). We found that Ad5-pIX-RFP-FF/NK2 demonstrated binding specificity to the cMet receptor. In addition, there was enhanced viral infectivity and virus replication compared with a non-targeted Ad vector. Although NK2 weakly induces cMet receptor activation, our results showed no receptor phosphorylation in the context of an oncolytic Ad virus. In summary, these results suggest that an oncolytic Ad retargeted to the cMet receptor is a promising vector for developing a novel cancer therapeutic agent.
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